applicazioni biomediche: terapie consolidate e utilizzi...
TRANSCRIPT
Radiazioni ionizzanti e non ionizzanti: Nuove Applicazioni Diagnostiche e Terapeutiche Sala Auditorium “Cosimo Piccinno” - Ministero della Salute Roma, 29 novembre 2019
Applicazioni biomediche: terapie consolidate e utilizzi innovativi
Carmela Marino
ENEA C.R. Casaccia
XI WORKSHOP INTERDISCIPLINARE FIRR
EMF radiation and some typical applications
Non Ionizing radiation
Non-ionizing radiation (NIR) refers to any type of electromagnetic radiation that does not carry
enough energy per quantum (photon energy) to ionize atoms or molecules—that is, to completely
remove an electron from an atom or molecule
Extremely Low Frequency (ELF) 0-3 kHz
Deep Brain Stimulation Transcranial
Magnetic Stimulation
Epidural Electrical Stimulation
Static (0 Hz) +ELF
Magnetic Resonance
Imaging
Transcranial Direct Current
Stimulation
Low frequency (1 Hz – 100 kHz)
Intermediate Frequency (300 Hz-100KHz)
Ultra Short High Voltage
Electric Pulses
Radio Frequency (100 kHz-300 GHz)
Microwave thermal ablation
Trans Cranial electromagnetic Stimulation for AD treatment
Hyperthermia
ELF-MFs application in Parkinson’s Disease (etiology)
By 2020, close to 1 million persons living in the United States will have a diagnosis of PD. PD is now widely recognized as not only movement disorder, but as a neuropsychiatric disorder, which includes cognitive impairment (both mild cognitive impairment and dementia), depression, and psychosis, and other relatively common and clinically significant psychiatric complications, like compulsive behaviors various anxiety symptoms, disorders of sleep and wakefulness, apathy, and fatigue
ELF-MFs application in Parkinson’s Disease (PD pathology)
Dopamine allows smooth, coordinated function of the body's muscles and movement
Parkinson's Disease (PD) is a neurodegenerative disorder pathologically characterized by 1. degeneration and loss (50-70%) of dopaminergic neurons in the substantia nigra pars compacta 2. presence of intracytoplasmic inclusions of α-synuclein and ubiquitin known as Lewy bodies (LBs)
Pilsl & Winklhofer, 2011
ELF-MFs application in PD: Deep Brain Stimulation (DBS)
DBS is a well-established functional neurosurgical technique that is used to treat a variety of neurological disorders. It consists in the implanting of electrodes in brain areas to electrically stimulate it and regulate abnormal impulses. In PD electrodes are usually implanted in subthalamic region, but recently also other areas are stimulated as globus pallidus and pedunculopontine nucleus.
PD treatment options have conventionally focused on dopamine replacement, resulting to be only partially effective in controlling the symptoms and totally useless to cure the pathology.
Globus pallidus
Subthalamic nucleus
Pedunculopontine nucleus
The current hypothesis is that pathologically altered and dysfunctional neuronal circuits, or circuitopathies, are treatable with DBS and that electrical stimulation can alter these neuronal circuits back to a more physiological state. Electrical excitability of neural tissue are determined by several factors:
The proportion of gray and white matter structures (i.e., cell bodies or axons)
The type of ion channels on the cell membrane of a soma or axon
The diameter and degree of myelination of axons
The orientation of axons in relation to the electrode
Electrode position and temporal aspects of of stimulation as some effects of DBS happen within
seconds, while others can take weeks to establish
The parameter of stimulation itself: single pulse or continuous stimulation, amplitude, voltage, polarity,
frequency, pulse width, pulse shape, rhythm
Basis of DBS
DBS neurochemical effects
Animal studies demonstrate an increase in DA release after DBS. In patients no release is observed.
NA might be involved in the mechanisms of action of DBS given the noradrenergic projections to the STN originating from the locus coeruleus. Depletion of NA and its metabolites within the limbic system has been implicated in both movement disorders and psychiatric pathology. DBS of different parts of brain have demonstrated to increase NA concentration, inducing an antidepressant effect
Serotonergic system dysfunction has been implicated in mood disorders. Recently serotonin has been demonstrated to modulate PD motor symptoms. Results about the effect of DBS on Serotonin need to be confirmed
In a STN-DBS cohort of PD patients, both levodopa administration and electrical stimulation caused a decrease in GABA content in the motor thalamus, suggesting similar mechanism of motor symptom alleviation. GABA levels were increased in the SNr during STN-DBS, which showed normalized reduced neural activity owing to decreased glutamatergic excitation. Since most DBS targets have both excitatory and inhibitory efferents and afferents, the overall effect on circuit behavior and phenotype is likely complex and is influenced by the relative distribution of these fibers
DBS increased capillary density, and increased expression of vascular endothelial growth factor (VEGF) and glial-derived neurotrophic factor (GDNF), led to the hypothesis that STN-DBS changes the microvasculature and causes sprouting of new more stables vessels compared to PD patients without DBS therapy
DBS: how do they work?
12
…we still don’t know, and we only have several hypotheses
Stimulatory or inhibitory effects Sometimes DBS stimulation increases the evoked potential, particularly in post synapsis. On the other side, DBS stimulation can induce an inhibition in neuron depolarization, blocking the action potential.
Local versus systemic effects It is now clear that the downstream effects of DBS are more systemic, involving excitation of axons both afferent and efferent to the site of stimulation.
Disrupting pathological oscillation. The oscillations that are normally detected in functioning neural networks are thought to facilitate dynamic communication and plasticity between spatially disparate populations of neurons. In PD pathological beta-band oscillatory activity is observed which correlates with PD symptoms. DBS disrupts and suppresses the beta-band oscillations reducing levels of bradykinesia and rigidity.
Cellular perspective At the cellular level, DBS directly activates astrocytes as well as neurons, causing release of various gliotransmitters, such as glutamate, d-serine and ATP66. Once stimulated, astrocytes contribute to the modulation of neuronal firing. Astrocytes also have direct effects on cerebral blood flow, causing either an increase or a decrease in neuronal activity by mediating neurovascular coupling
Beyond basal ganglia to cortex Recent investigations have shown that acute DBS exerts a marked influence on the cortex by reducing excessive coupling between beta oscillations and broadband activity. Therefore, although the site of DBS current delivery is at the basal ganglia, its mechanism of neuromodulatory action seems to be at least partly mediated (antidromically or orthodromically) remotely at the cortex.
Neuroprotection Evidence is accumulating that DBS confers protection on dopaminergic cells. So DBS would not only be a therapeutic tool, but also would slow down the progression of the pathology.
Transcranial Magnetic Stimulation (TMS)
Lines of magnetic flux
magnetic coil consisting of small number of copper wire tightly wound in an insulating material
Induced current in brain. Magnetic stimulation induces an electric current in brain, whose direction will be parallel but opposite to the current in the primary coil, which his the source of the magnetic field. This induced electric field will have effect on pyramidal and cortex neurons
TMS is a powerful technique to non-invasively stimulate the human brain. TMS uses short-lasting, strong electric currents delivered through a copper wire coil to generate a rapidly changing high-intensity magnetic field.
Single pulses can evoke electromyographic responses providing an opportunity to quantify changes in cortical activation
TMS brain effects
Repetitive TMS (rTMS) have different effect than single pulse stimulation. They can either enhance (5-20 Hz, high frequency stimulation) or suppress (approximately 0.2-1 Hz, low-frequency stimulation) cortical activity and modulate excitability beyond the duration of the applied trains, depending on the frequency applied.
Chervyakov et al., Front. Hum. Neurosci. 2015
Effects of rTMS on cells
epigenome
LTP (induced by high frequency) enhances synaptic strength and can persist for several days, weeks, or months, whereas LTD (induced by low frequency) results in the long-term reduction of synaptic strength
Brunoni et al., Braz J Psychiatry. 2019
Increased neurogenesis and differentiation of DA neurons was observed in animal studies, which correlated with improvements of motor symptoms
rTMS applications in brain diseases
“Repetitive transcranial magnetic stimulation therapy for motor recovery in Parkinson's disease: A Meta‐analysis”
Yang et al., Brain Behav. 2018;8(11):e01132 rTMS might be helpful in improving the motor deficits of PD. High frequency rTMS appears more significant effect than
Low Frequency‐rTMS Stimulation over M1 shows better efficacy than other
stimulation sites; bilateral stimulation is more effective than unilateral stimulation; multi‐session higher dosage of pulses (total 18,000–20,000 pulses) are associated with better motor outcome.
The effect of rTMS appears to be long‐lasting and unaffected by the patient’s medication state.
Major Depressive Disorders (MDD) rTMS is a first-line treatment for patients in whom at least one antidepressant trial has failed. rTMS is not so effective as Electroconvulsive therapy for treating MDD, but the combination with drugs can improve the efficacy of rTMS. This stimulation can also improve the cognitive tasks involved in the pathophysiology of depression.
Schizophrenia, obsessive compulsive disorders, anxiety, stress, addiction
Data show that there are not unambiguous results, so other studies are necessary to address the question Brunoni et al., Braz J Psychiatry 2019
TMS applications in stroke
Stroke, or cerebrovascular accident, represents the third leading cause of death and one of the most common sources of disability worldwide. Motor deficits after stroke have been given particular attention; however, other types of deficits are also relevant such as communication skills, swallowing abilities and attention
Motor function Both high and low frequency TMS stimulation applied to both sides of the brain have been demonstrated effective in motor recover in acute and subacute stroke (Schulz et al., Neuropharmacology 2013).
Aphasia The brain area stimulated is the inferior frontal gyrus. Improvements in aphasia recovery with the application of rTMS, mainly in picture naming. The majority of the studies on aphasia recovery focused on chronic stroke patients; 62% of the included research recruited patients that had had the stroke event more than 1 year before. The stable baseline condition, in the chronic phase, favors a more objective assessment of the TMS effects. However, application of TMS in acute seems to be more effective (Dioniso et al., Cerebrovasc Dis 2018).
Disphagia There is a great inter-study variability both on the stimulation area and on the design of protocols. All but one of the included studies demonstrated qualitatively good results in improving dysphagia, and were able to describe that patients recovered swallowing ability into different extents. All the stimulations were performed in acute phase, which makes difficult to understand if the recover was effectively due to TMS (Dioniso et al., Cerebrovasc Dis 2018).
Transcranial direct current stimulation (tDCS)
tDCS is a technique that delivers a low electric current to the scalp. A fixed current between 1 and 2 mA is typically administered by applying a positive (anodal) or negative (cathodal) current via electrodes to an area, facilitating the depolarization or hyperpolarization of neurons, respectively. The current delivered by tDCS is not considered strong enough to trigger an action potential in a neuron, but sufficient to alter both the excitability and spontaneous activity of neurons
Brunoni et al., Braz J Psychiatry. 2019
Physiological mechanisms of tDCS
Direct current stimulation aims to directly modulate neuronal resting potentials and to alter the state of excitability without inducing a supra-threshold neuronal membrane depolarization, resulting in generation of an action potential. If a neuronal membrane is depolarized by a DC current, an action potential is induced; if it is hyperpolarized, neuronal excitability is reduced. The target cortical area to be stimulated will depend on the reason of stimulation. Primary motor
cortex M1
Ripoll Rozisky et al., 2015
Application of tDCS in brain diseases
Azheimer’s Disease
Attention Neuropsychiatric
Symptoms
Memory
Alzheimer type dementia
Memory
behavior and functional activity
Studies ongoing
Parkinson’s Disease
Motor symptoms
stroke
motor function
Mixed results
Hemineglect Promising but
few results
Pain management
Promising results, but they need to be corroborated
DC stimulation and spinal cord injury (SCI)
SCI is damage to the spinal cord that causes temporary or permanent changes in its function. According to the National Spinal Cord Injury Statistical Center, there are 12,500 new cases of SCI each year in North America (Symptoms may include loss of muscle function, sensation, or autonomic function in the parts of the body served by the spinal cord below the level of the injury. It can be complete, with a total loss of sensation and muscle function, or incomplete, meaning some nervous signals are able to travel past the injured area of the cord.
The initial mechanical forces delivered to the spinal cord at the time of injury is known as primary injury. Four main characteristic mechanisms of primary injury have been identified that include: (1) Impact plus persistent compression; (2) Impact alone with transient compression; (3) Distraction; (4) Laceration/transection
Secondary injury in SCI
Secondary injury begins within minutes following the initial primary injury and continues for weeks or months causing progressive damage of spinal cord tissue surrounding the lesion site. Secondary injury can be temporally divided into acute, sub-acute, and chronic phases.
acute phase
sub-acute phase
chronic phase
Current therapies in SCI
At present, activity-based therapies are the only medical practices that can be used to enhance recovery. The volitional production of active movements during training promotes reorganization of neuronal pathways and thereby augments recovery. However, the most affected patients, who fail to produce active movements voluntarily, experience minimal benefits from these therapies. This situation has prompted the development of multifaceted neurotechnologies: such as lower limb exoskeletons, bodyweight support systems, functional electrical stimulation of muscles, and spinal cord neuromodulation therapies, all of which share the same goal: to enable patients to sustain active movements during training to enhance the reorganization of neuronal pathways.
lower limb exoskeletons
bodyweight support systems
electrical stimulation of muscles
All these therapies share the same goal: to enable patients to sustain active movements during training to enhance the reorganization of neuronal pathways
DC stimulation improves neurigenesis and nerve regeneration
Koppes et al., Journal of neural engineering, 2011
NGF
rat dorsal root ganglia neurons 10 mV/mm 100 mV/mm
CTR The ability of electric field to induce neuritogenesis is well known and has been proven since several years
Anderson et al., Nature 2018
Thanks to this capacity, DC stimulation is also able to induce nerve regeneration
Rat spinal cord lesioned
EES seems to be the proper therapy to obtain the better results in Sci. This stimulation, not only enables the brain to exploit spared but functionally silent descending pathways in order to produce movements of paralysed limbs, but also improves the ability of the spinal cord to translate task-specific sensory information into the muscle activity that underlies standing and walking
Epidural electrical stimulation (EES) in SCI
A 16-electrode array is surgically implanted on Dura of lesioned area
spinal cord stimulator implanted surgically in the anterior abdominal wall The electric field applied is an ELF signal
(from 2 up to 50 Hz) and the amplitude is set on the basis of the stimulation necessary to activate muscles response as detected by EMG recording electrodes
EES stimulation can induce a recovery in SCI patients
“Recovery of Over-ground walking after chronic motor complete SCI” Angeli et al. N Engl J Med 2018
Four participants with traumatic, motor complete spinal cord injury, meaning the absence of voluntary movement below the level of injury with or without some preserved sensation
2 Hz stimulation 20 days after the stimulator implantation
training with the epidural stimulator turned on
Two of the four participants were able to walk over ground with assistive devices after intensive physical training with electrical stimulation of the lower spinal cord. All four participants could not do these actions in trials when the stimulator was off.
EES stimulation restores walking in SCI patients
Within one week, re-established adaptive control of paralysed muscles during overground walking.
Locomotor performance improved during rehabilitation.
After a few months, participants regained voluntary control over previously paralysed muscles without stimulation and could walk or cycle in ecological settings during spatiotemporal stimulation
trains of spatially selective stimulation to the lumbosacral spinal cord with timing that coincided with the intended movement
Low‐energy low‐frequency pulsed electromagnetic fields (PEMF) and brain
PEMF have been demonstrated particularly efficacy in the treatment of a variety of inflammatory disorders including pseudoartrosis, joint disease, complications related to diabetes mellitus. In brain the action of PMF has been explored in several diseases and injuries :
Modulate neuroinflammation TNF-α, NFκB, IFN-γ
Il-4, IL-10
Stimulate nerve regeneration
Regulating developmental and regenerative cell growth and guidance
Increasing neuritogenesis Differentiating stem cells
(MSC) transplanted in lesioned area
SCI REPAIR
improve the ability of learning and memory
Increase IGF2 expression
AD LIKE DEMENTIA
activation of the BDNF/TrkB/Akt signaling pathway. pro-survival proteins pro-apoptotic proteins and inflammatory mediators
STROKE Neuroprotective effect
Ultra short electric pulses: emerging technology in brain disease and injuries?
Microsecond (μsec) and nanosecond (nsec) pulses are defined as very short high intensity electric pulses
which present great potential for the destabilization of intracellular structures.
The resulting current from the application of these pulses on cells causes accumulation of electrical charges
at the cell membrane and consequently a voltage across the membrane. If the membrane voltage exceeds
a critical value, structural changes in the surface membrane occur that cause pore formation/increased
permeability (electroporation).
If the membrane voltage is not excessive and the duration of the pulse is limited, the increased membrane
permeability can be reversible and the cell survives, an effect that is used for electrochemotherapy and gene
delivery into cells.
The time required to charge the surface membrane is dependent upon the electrical parameters of both the
cell and the medium in which it is suspended. μsec nsec
Ultra short electric pulses effects on cells
Microsecond pulses
ELECTROPORATION: These pulses are
able to permeabilize cellular membranes.
Using one or several pulses can change
the cell membrane structure allowing the
access to the cell cytosol of molecules that
cannot cross the plasma membrane under
normal conditions.
Ca++ flux: from the outside and
intracitoplasmatic organelles is induced
NO OR LESS IMPACT ON CELL
MEMBRANE: only the ones which has
longer duration can induce the formation
of nanopores.
LARGER EFFECT ON CELL INTERIOR than
longer pulses (micro- and millisecond
pulses).
Nanosecond pulses
MEDICAL APPLICATION
ELECTROCHEMOTHERAPY
Calcium electroporation to induce tumor necrosis.
Tumor cell apoptosis induction
Drug and DNA delivery
Ultra short electric pulses current medical application
Ultra short electric pulses can modulate Ca++ flux inside cells
Ca++ is an ion that only crosses the plasma and ER membranes through channel proteins. Applying PEFs to cells in a medium containing Ca++ allows this ion to entry from the cell outside, and, if the electric field amplitude and pulse duration are high enough, Ca++ is released from the cell inner stores, such as endoplasmic reticulum
Mesenchimal stem cells
Pulse applied at 630s
100 μsec 300 V/cm
100 μsec 950 V/cm
Spostaneous Ca++ oscillations
According to the pulse(s) electric field amplitude, it is possible to generate a supplementary calcium spike with properties close to those of calcium spontaneous oscillations, or, on the contrary, to inhibit the spontaneous calcium oscillations for a very long time compared to the pulse duration
Hanna et al., 2017
Ca++ is a major second messenger in neurons
During neurogenesis cellular Ca++ signals regulate nearly every aspect of neural development including neural induction, proliferation, migration, and differentiation
Toth et al., Cell Calcium, 2016
Ca++
Neuronal excitability
Release of Neurotransmitter
Synaptic plasticity
Role of Ca++ signal in mature neurons
abnormal Ca++ signaling
Is it possible to modulate neurons Ca++ signaling through PEF?
Enea’s ongoing results on SH-SY5Y and on MSC μsec pulses stimulation nsec pulses
stimulation
PVDM “pools”
Time (min)
Fluo
resc
ence
inte
nsity
Ca++ flux
• No influence on cell proliferation • No influence on cell death • No influence on redox homeostasis • Modulation of immediate early genes egr1 and c-fos • Modulation of differentiation markers? ongoing…..
Che cosa è l’ipertermia
L’ipertermia è una tecnica di trattamento terapeutico dei tumori, utilizzata da diversi anni in oncologia medica in combinazione con chirurgia, chemioterapia e/o radioterapia.
La tecnica prevede una distribuzione accurata di calore nella zona da trattare con l’obiettivo di ottenere nel tumore un incremento di temperatura fino a 41–45 °C per circa 60 minuti.
In tal modo è possibile incrementare l’efficacia degli agenti chemio- e radio-terapici sfruttando l’azione sensibilizzante del calore sulle cellule tumorali.
Fin dai primordi della medicina si usava trattare piccoli tumori non ulcerati con il ferro incandescente (Ramajama 2000 a.C; Ippocrate 400 a.C; Galeno 200 d.C).
La prima documentata evidenza che le temperature elevate potevano avere un effetto terapeutico sui tumori è attribuita a Bush, che nel 1866 riferiva della scomparsa di un sarcoma della faccia, istologicamente documentato.
Casi simili furono successivamente descritti da un chirurgo americano, Wiliam B. Coley (1893), il quale, alla fine del secolo scorso, trattò diversi pazienti oncologici con una tossina estratta da batteri (tossina di Coley) per indurre elevati stati febbrili.
Uno dei pionieri dell’ipertermia locale indotta dall’esterno fu un ginecologo svedese (Westermark 1898), che applicò l’ipertermia in un carcinoma avanzato della cervice uterina. Egli usò una spirale metallica, attraverso la quale veniva fatta circolare dell’acqua calda, a diretto contatto con il tumore.
Ipertermia nella storia
Basi biologiche dell’ipertermia
L’ipertermia è di per sé citotossica
Se si osserva la frazione di crescila di cellule in coltura in funzione del tempo e della temperatura, si possono notare delle curve simili a quelle evidenziabili con le radiazioni ionizzanti, con o senza una spalla iniziale, seguita da un decremento esponenziale (Dewey et al. 1977).
This difference above and below 42.5-43°C has been observed on a large variety of mammalian systems - independently from the different heat sensitivities of the various cell types- and has therefore a supposedly general validity.
Survival kinetics above and below 42.5-43°C has been usually described by an Arrhenius plot, where the log 1/Do, that is, a measure of the slope of the exponential portion of the survival curve is plotted against 1/T (the absolute temperature).
M. W. Dewhirst et al, Basic principles of thermal dosimetry and thermal thresholds for tissue damage from hyperthermia, Int. J.
Hyperthermia, 19, 3, 267-294
Comparison of Arrhenius plot for a series of rodent and
human cell lines, derived from cell survival curve data. The plot consider the rate of cell
killing on the exponential portion of the curves.
Thermotolerance
Surviving fraction of CHO-cells at 43°C, preheated at 40 °C for various periods of time (Jung H, Radiat Res 1982)
‘Thermotolerance’, is principally reversible. It is partially based on the induction of heat-shock proteins (HSP) and other post-transitional adaptation processes (e.g. cell cycle arrest in the G2-phase, changes in cell metabolism).
• It is now clear that in actual tumors in situ, an increase in blood flow and consequent increase in oxygenation by heating may significantly enhance the response of tumors to radiotherapy to a greater degree than any inhibition of thermal killing related to the occurrence of thermotolerance.
• Further, heat-induced radiosensitization is not subject to thermotolerance.
• Under normal heating conditions used in the clinic, thermotolerance may not be induced to any significant degree.
Razionale dell’associazione radioterapia + ipertermia (1)
L’ipertermia come unico trattamento permette di ottenere in clinica risposte solo parziali in circa il 20% dei pazienti (Sannazzari et al., 1986).
Esistono però numerosi dati sperimentali e clinici che dimostrano un effetto sinergico con le radiazioni ionizzanti.
Soprattutto in presenza di grosse masse neoplastiche la radioterapia da sola non riesce a ottenere la remissione completa, a causa di diversi fattori: • radioresistenza intrinseca: • popolazione cellulare eterogenea; • dose limitante, legata ai tessuti sani circostanti: • volume troppo grande per una terapia radicale; • scarsa vascolarizzazione e conseguente ipossia.
Razionale dell’associazione radioterapia + ipertermia (2)
L’ipertermia interagisce con le radiazioni per mezzo di diversi meccanismi: • citotossicità diretta (denaturazione delle membrane proteiche e citoplasmatiche) • alterazioni della perfusione sanguigna (ossigenazione) e del micro-ambiente tumorale
(acidosi) • sinergismo con le radiazioni (riduzione della riparazione del danno sub-letale al DNA)
Inoltre si ipotizzano effetti dell’ipertermia su: • espressione della proteina di riparazione del danno termico (HSP) • induzione e regolazione dell’apoptosi • modulazione della resistenza ai farmaci (maggiore captazione - o minore eliminazione? - del
farmaco all’interno della cellula) Diversi fattori influenzano l’interazione dell’ipertermia con le radiazioni ionizzanti: • tempo di riscaldamento • temperatura raggiunta • sequenza dei trattamenti • intervallo fra i trattamenti • numero di trattamenti • dimensioni del tumore • vascolarizzazione
Van Rhoon et al 2016
Protonterapia combinata con ipertermia
Slow-growing tumours with a lower α/β ratio, e.g. prostate, melanoma, sarcoma, breast etc., as such tumours with lower α/β ratio are usually radio-resistant and are best treated with hypofractionated treatment regimens as used in most 12C-ion therapy treatment protocols.
Protonterapia combinata con ipertermia Studi clinici in corso
Combined Hyperthermia and Protonterapy
Datta et al, Int J Hyperthermia, 2014; 30(7): 524–530
Background
• The glioblastoma multiforme (GBM) is the most aggressive brain tumor with poor survival despite the many therapeutic strategies explored.
• Conventional radiotherapy remains the main treatment for GBM
• Several clinical trials suggest that hadrontherapy (especially 12C-ion) could be particularly promising
• Hyperthermia (HT) has been considered to be the most powerful way of sensitizing ionizing radiation
• The hypothesis that hyperthermia coupled with proton (P) irradiation could mimic 12C-ion therapy is currently investigated.
ESHO 2018 Conference
ESHO 2018 Conference
ESHO 2018 Conference
Clonogenic survival assay (U-251 cell-line)
HT+PT vs. HT+X-rays
Termoablazione a microonde
L’energia elettromagnetica a frequenze delle microonde (915 MHz, 2.45 GHz, …) è impiegata per ottenere un elevato incremento di temperatura (> 55-60°C) nella zona da trattare tale da indurre una necrosi coagulativa pressoché istantanea
Trattamenti clinici: • aritmie cardiache • disturbi endometriali • tumori (radiologia interventistica)
Tecnica minimamente invasiva (antenne interstiziali)
Ottenibili ablazioni con diametro fino a 5 cm (ago singolo/singola ablazione) Lesioni più grandi possono essere trattate con applicatori multipli o ablazioni sovrapposte
Oltre 15.000 interventi clinici praticati in Europa Occidentale ogni anno
Oltre 100.000 interventi annui a livello mondiale
MW power generator
cooling system
coaxial cable
MW antenna
applicator
carbonized zone (>100ºC)
coagulated zone (60ºC-100ºC)
Il problema clinico
Obiettivi: ➯ ottenere l’opportuno incremento di temperatura (> 60°C) in
un’area ben definita (lesione da trattare + margine sicurezza) ➯ Trattamento mini-invasivo (tollerabilità, riduzione effetti collaterali)
Procedura: • Acquisizione di immagini (TAC/RM) della zona da trattare • Determinazione del bersaglio (lesione tumorale) • Definizione del protocollo di trattamento (tempo-potenza) • Targeting applicatore (sotto guida ECG/TAC) • Verifica (TAC/RM) e eventuale ripetizione del trattamento
Criticità: • Approccio empirico (standardizzazione protocolli) • Controllo in tempo reale (metodi non invasivi)
Take home messages
Terapie non invasive: pulses (anche per veicolare macromolecole/vaccini/farmaci ) HT vs RT vs PT: direct cell killing, selective cytotoxicity of the radioresistant hypoxic cells, ability to kill radioresistant S phase cells and inhibition of radiation induced DNA damage repair (direct effects on major DNA repair factors), Damage signaling, checkpoints, cell cycle progression and apoptosis.